Rapid alterations of cell cycle control proteins in human T lymphocytes in microgravity

被引:0
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作者
Cora S Thiel
Katrin Paulsen
Gesine Bradacs
Karolin Lust
Svantje Tauber
Claudia Dumrese
Andre Hilliger
Kathrin Schoppmann
Josefine Biskup
Nadine Gölz
Chen Sang
Urs Ziegler
Karl-Heinrich Grote
Frauke Zipp
Fengyuan Zhuang
Frank Engelmann
Ruth Hemmersbach
Augusto Cogoli
Oliver Ullrich
机构
[1] University of Zurich,Institute of Anatomy, Faculty of Medicine
[2] University of Muenster,Institute of Medical Physics and Biophysics
[3] Universitaetsplatz 2,Department of Machine Design, Engineering Design and Product Development, Institute of Mechanical Engineering, Otto
[4] Otto-von-Guericke-University Magdeburg,von
[5] University of Zurich,Guericke
[6] KEK GmbH,University Magdeburg
[7] Beihang University,Institute of Molecular and Clinical Immunology
[8] University Medical Center of Johannes Gutenberg-University Mainz,Center for Microsocopy and Image Analysis
[9] University of Applied Science Jena,School of Biological Science and Medical Engineering
[10] Institute of Aerospace Medicine,Clinic for Neurology
[11] Zero-G Life Tec,German Aerospace Center (DLR)
[12] University of Zurich,Zurich Center for Integrative Human Physiology (ZIHP)
关键词
Adaptive immunity; spaceflight; signal transduction; gravisensitivity;
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摘要
In our study we aimed to identify rapidly reacting gravity-responsive mechanisms in mammalian cells in order to understand if and how altered gravity is translated into a cellular response. In a combination of experiments using "functional weightlessness" provided by 2D-clinostats and real microgravity provided by several parabolic flight campaigns and compared to in-flight-1g-controls, we identified rapid gravity-responsive reactions inside the cell cycle regulatory machinery of human T lymphocytes. In response to 2D clinorotation, we detected an enhanced expression of p21 Waf1/Cip1 protein within minutes, less cdc25C protein expression and enhanced Ser147-phosphorylation of cyclinB1 after CD3/CD28 stimulation. Additionally, during 2D clinorotation, Tyr-15-phosphorylation occurred later and was shorter than in the 1 g controls. In CD3/CD28-stimulated primary human T cells, mRNA expression of the cell cycle arrest protein p21 increased 4.1-fold after 20s real microgravity in primary CD4+ T cells and 2.9-fold in Jurkat T cells, compared to 1 g in-flight controls after CD3/CD28 stimulation. The histone acetyltransferase (HAT) inhibitor curcumin was able to abrogate microgravity-induced p21 mRNA expression, whereas expression was enhanced by a histone deacetylase (HDAC) inhibitor. Therefore, we suppose that cell cycle progression in human T lymphocytes requires Earth gravity and that the disturbed expression of cell cycle regulatory proteins could contribute to the breakdown of the human immune system in space.
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